1. Combined loss of MPG and ATM sensitizes pGBM cells to temozolomide (TMZ) in vivo.
Combined loss of MPG and ATM sensitizes pGBM cells to temozolomide (TMZ) in vivo. A, immunoblotting of SJG2 cells demonstrating effective MPG, ATM, or dual knockdown. B, the Kaplan–Meier survival curve analysis of intracranially injected SJG2 cells expressing control shRNA, MPG shRNA, ATM shRNA, or dual knockdown into NOD/SCID mice. C, the Kaplan–Meier survival curve analysis of intracranially injected SJG2 cells expressing control shRNA, MPG shRNA, ATM shRNA, or dual knockdown into NOD/SCID mice treated with temozolomide (65 mg/kg/5 days). D, quantification of Ki67 staining in mice (n = 3 mice per group) from C. E, the Kaplan–Meier survival curve analysis of intracranially injected SJG2 cells into NOD/SCID mice treated with vehicle, temozolomide (TMZ; 65 mg/kg/5days), methoxyamine (MA; 100 mg/kg/5 days), or both temozolomide + methoxyamine. F, quantification of Ki67 staining in mice (n = 3 mice per group) from E. G, the Kaplan–Meier survival curve analysis of an orthotopic PDX mouse model from pGBM462 cells. A total of 20 mice were injected with 5 per each treatment arm: vehicle, temozolomide (65 mg/kg/2 weeks), methoxyamine (100 mg/kg/2 weeks), or both temozolomide + methoxyamine (65 mg/kg temozolomide and methoxyamine 100 mg/kg for 2 weeks). H, H&E staining of represented tumors mice from each treatment arm confirmed high-grade glioma/GBM morphology. Scale bar, large insets at 500 μm and small magnified insets at 25 μm. N, normal mouse brain; T, xenograft tumor growth. E and G, mice were treated upon confirmation of tumor by T2-MRI. *, P < 0.05; **, P < 0.01.
Sameer Agnihotri et al. Cancer Discovery 2014;4:
©2014 by American Association for Cancer Research